ORYX Translational Medicineoryx-medicine.com/fileadmin/user_upload/uploads/News/Publications/... ·...
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ORYX – Overview
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ORYX GmbH & Co. KG (ORYX) is a privately held company for translational oncology founded in 2007 and located in Baldham/Munich, Germany
ORYX bridges the gap for new cancer therapies between leading academic research institutions and the pharmaceutical industry
ORYX is the exclusive licensee of three premier cancer immunotherapy substances of the German Cancer Research Center (DKFZ) and the University of Heidelberg
ORYX has successfully developed these substances in clinical phase I/IIa trials, has obtained compelling safety and efficacy data in these clinical trials, and is now looking into partnering these substances for the pivotal trials
ORYX – Pipeline
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Cancer Immunotherapy
Substances
Mode of Action
Current Cancer
Indications
Pre-Clinical Clinical Development
MicOryx
VicOryx
ParvOryx
Synthetic frameshift
peptides vaccine
Synthetic humancyclin-dependentKinase inhibitorpeptide vaccine
Wild-type ratoncolytic virus
Concurrent vaccination & chemotherapy
Colorectal
Cervical Head & Neck
GBM
PDAC
Phase I / IIa completed
Phase I / IIa completed
Phase I / IIa completed
Phase I / IIaongoing
Phase I / IIa ongoing
POC / Toxicology
Phase I Phase II Phase III
Several cancers arise from the lack of DNA mismatch repair (MMR), resulting in the
accumulation of single deletions or insertions at coding microsatellites (MSI-H mutations)
Cancers with MSI-H mutations include:
10-15% of colorectal cancers
20-25% of endometrial cancers
25-30% of upper urinary tract cancers
15-20% of gastric cancers
5-10% of pancreatic cancers
MSI-H mutations lead to the expression of frameshift peptides (FSPs)
FSPs are tumor specific antigens which are constantly expressed
In patients with MSI-H colorectal cancer a natural humoral and cellular immune response against FSPs
is found, which demonstrates that FSPs are recognized by the immune system and can trigger an immune response
MicOryx – Rationale
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Results
Primary Objective: Safety
• 22/22 patients (100%)
Secondary Objective: Efficacy
• Specific immune responses against FSPs in 21/22 patients (95,5%)
• Stable Disease in stage III and IV patients
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Trial design
Single center, two part open label, prospective study
• 1st part 6 patients, 2nd part 16 patients (n = 22)
• UICC stage III/IV MSI-H colorectal cancer
Total of 12 s.c. applications with three FSPs one time/week for four consecutive weeks, followed by a four week rest period (one cycle) for a total of three cycles
Monitoring of toxicity, immune response (including DTH), and tumor response
Subcutaneous injection of FSPs and Montanide ISA 51 VGStudy Week
1 2 3 4 9 10 11 12 17 18 19 20 25
MicOryx 01 – Clinical Phase I/IIa – completed
In many solid cancers the cyclin-dependent kinase inhibitor p16INK4a is expressed
p16INK4a positive cancers include:
20-30% of breast cancers
60-70% of small cell lung cancers
90-100% of HR-HPV associated cancers, e.g.cervical cancer, head and neck cancer, anal and vulvar cancer, vaginal and penile cancer
In cancer cells, p16INK4a is a tumor antigen which is constantly expressed as an early consequence
of cell transformation
In normal cells, p16INK4a is rarely expressed and leads to immediate senescence
In patients with HR-HPV associated cancers a natural humoral and cellular immune response against p16INK4a can be found, which indicates that p16INK4a is recognized by the immune system
and can trigger an immune response
VicOryx – Rationale
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VicOryx 01 – Clinical Phase I/IIa - completed
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Trial design
Single center, two part open label, prospective study
• 1st part 10 patients, 2nd part 16 patients (n = 26)
• UICC stage III/IV, advanced HR-HPV- and p16INK4a
positive cervix, vulvar, vaginal, penile, anal or head and neck cancer
Total of 12 s.c. applications with a specific p16INK4a
peptide one time/week for four consecutive weeks, followed by a four week rest period (one cycle) for a total of three cycles
Monitoring of toxicity, immune response (including DTH), and tumor response
Subcutaneous injection of p16 and Montanide ISA 51 VGStudy Week
1 2 3 4 9 10 11 12 17 18 19 20 25
Results
Primary Objective: Safety
• 26/26 patients (100%)
Secondary Objective: Efficacy
• Specific immune responses against p16INK4a in 18/26 patients (69,2%)
• Stable Disease in stage III and IV patients
VicOryx 01 – Clinical Phase I/IIa - completed
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Progression-free survival by overall Immune response Overall Survival by overall immune response
Significantly prolonged PFS (p = 0,003) and OS (p = 0,0018)
VicOryx 02 – Clinical Phase I/IIa - ongoing
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Trial design
Single center, open label, prospective study
• On concurrent cisplatin-based chemotherapy combined with specific p16INK4a peptide vaccination,
10 patients
• UICC stage III/IV, advanced HR-HPV- and p16INK4a
positive cervix, vulvar, vaginal, penile, anal or head and neck cancer
Total of 12 s.c. applications with a specific p16INK4a
peptide one time/week for four consecutive weeks, followed by a four week rest period (one cycle) for a total of three cycles
• Vaccination is applied one week before the initiation or continuation of cisplatin-based chemotherapy
• All patients included
Results
Primary Objective:
• Feasibility of vaccination during chemotherapy
• Specific immune response against p16INK4a
Secondary Objective:
• Safety, PFS, OS
• Tumor response according to RECIST
Combined therapy so far shows excellent safety and tolerability
ParvOryx – Synopsis
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PotentialsCharacteristics
Wild type DNA virus
Excellent safety profile
it. and/or iv.
No prior immunity in humans
Repeated it. and/or iv. application
Oncolysis and bystander effect
• Passes blood brain barrier• Potential to be armed with tumour specific siRNAs
• Not pathogenic for humans• Lyses only tumour cells• No effect on normal tissue
• H-1PV antibodies appear in dose dependent manner
• Potential to vaccination
• High H-1PV susceptibility in many cancers• Potential to change tumor microenvironment• Combined modalities
• Potential to local and systemical administration
Virus Type
Safety
Application
Immunity
Booster
Efficacy
ParvOryx 01 - Clinical Phase I/IIa - completed
Trial design
Single center, open label, prospective, dose escalating study
• 1st group (it) 12 patients, 2nd group (iv) 6 patients (n = 18)
• UICC Stage IV
• progressive primary or recurrent glioblastoma multiforme
It: half of the dose in the tumor, half of the dose in the wall of the resection cavity
Iv: half of the dose in 5 consecutive injections, half of the dose in the wall of the resection cavity
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Results Immune response
Primary Objective: Safety Strong cellular immune response against
• 18/18 patients (100%) glioma and viral proteins (bystander effect)
Secondary Objective: Efficacy• PFS ≥ 6 month: 33% / 10%• OS ≥ 6 month: 80% / 40%
ParvOryx 02 – Clinical Phase I/IIa - ongoing
Trial design
Single center, open label, prospective, dose escalating study, 7 Patients
• UICC stage IV metastatic inoperable pancreatic cancer
iv. administrationit. administration in single liver metastases
Results
Primary Objective: Safety
Secondary Objective:PFS, OSAnti-tumor effects
• Specific cellular and humoral immune responses
• Tumor infiltration
• Metastatic necrosis
• Virus activity in the tumor tissue
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ParvOryx – Relapsing GBM Compassionate Use Program
Design
6 patients from ParvOryx 01 requested another H-1PV application on the basis of a compassionate use agreement after resection of tumor recurrence
• After tumor resection virus was reapplied in the wall of the resection cavity • All patients received the same virus dose of 5x108 PFU
1. Rec.
Tumor res. + 1. Virus appl.
2. Rec.
Tumor res. + 2. Virus appl.
3. Rec./Death
ParvOryx 01 PFS1 Compassionate use program PFS2
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Results Results OS
Median PFS 1 = 6.4 Median OS (1. Virus appl. > 3. Rec./Death) = 37.9Median PFS 2 = 13.7 Historical data = 15 - 17 In 6/6 patients PFS2 was longer than PFS1
This is breaking the PFS paradigm in GBM
Disclaimer
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This Presentation includes and is based, inter alia, on forward-looking information and statements that are subject to risks and uncertainties that could cause actual results to differ. These statements and this Presentation are based on current expectations, estimates and projections, which generally are identifiable by statements containing words such as ”expects”, ”believes”, ”estimates” or similar expressions. Important factors that could cause actual results to differ materially from those expectations include, among others, general economic and industry conditions in markets which are expected to be major markets for ORYX products, as well as risks and uncertainties related to product development, regulatory approvals, commercial partnerships, the outcome of intellectual property rights litigation and the competitive situation.
Although ORYX believes that its expectations and the Presentation are based upon reasonable assumptions, it can give no assurance that those expectations will be achieved or that the actual results will be as set out in the Presentation. ORYX is making no representation or warranty, expressed or implied, as to the accuracy, reliability or completeness of the Presentation, and neither ORYX nor any of its directors, officers or employees will have any liability to you or any other persons resulting from your use of the information contained herein.
This presentation was prepared for the 2016 BIO International Convention in San Francisco on June 6-9, 2016. The slides should be read and considered in connection with other information provided by the company.
Marktplatz 1
85598 Baldham, Germany
ORYX – Partnering Opportunities
Phone: +49-8106-21 311-0
Fax: +49-8106-21 311-66
E-mail: [email protected]
ContactORYX GmbH & Co. KG
www.oryx-medicine.com